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恒河猴淋巴组织的功能和形态发育以及免疫调节和效应功能:分泌细胞因子的细胞、分泌免疫球蛋白的细胞和CD5(+) B-1细胞在胎儿发育早期就出现了。

Functional and morphological development of lymphoid tissues and immune regulatory and effector function in rhesus monkeys: cytokine-secreting cells, immunoglobulin-secreting cells, and CD5(+) B-1 cells appear early in fetal development.

作者信息

Makori Norbert, Tarantal Alice F, Lü Fabien X, Rourke Tracy, Marthas Marta L, McChesney Michael B, Hendrickx Andrew G, Miller Christopher J

机构信息

California National Primate Research Center, Center for Comparative Medicine, University of California, Davis, California 95616-8542, USA.

出版信息

Clin Diagn Lab Immunol. 2003 Jan;10(1):140-53. doi: 10.1128/cdli.10.1.140-153.2003.

Abstract

Little is known regarding the timing of immune ontogeny and effector function in fetal humans and nonhuman primates. We studied the organization of lymphocyte and antigen-presenting cell populations in developing lymphoid tissues of rhesus monkey fetuses during the second and third trimesters (65 to 145 days of gestation; term = 165 days). Immunoglobulin-secreting and cytokine-secreting cells were detected at day 80. The thymus, spleen, lymph nodes, and intestinal mucosa were examined for cells expressing CD3, CD5, CD20, CD68, p55, and HLA-DR. In the spleens of 65-day-old fetuses (early second trimester), the overwhelming majority of total lymphocytes were CD5(+) CD20(+) B-1 cells. The remaining lymphocytes were CD3(+) T cells. By day 80, splenic B and T cells were equal in number. Intraepithelial CD3(+) CD5(-) T cells and lamina propria CD20(+) CD5(+) B cells were present in the intestines of 65-day-old fetuses. By day 80, numerous CD20(+) CD5(+) B cells were present in the jejunums and colons and early lymphocyte aggregate formation was evident. The spleens of 80- to 145-day-old fetuses contained immunoglobulin M (IgM)-secreting cells, while IgA-, IgG-, interleukin-6-, and gamma interferon-secreting cells were numerous in the spleens and colons. Thus, by the second trimester, the lymphoid tissues of the rhesus monkey fetus have a complete repertoire of properly organized antigen-presenting cells, T cells, and B cells.

摘要

关于人类胎儿和非人灵长类动物免疫个体发生的时间以及效应功能,我们所知甚少。我们研究了恒河猴胎儿在妊娠中期和晚期(妊娠65至145天;足月为165天)发育中的淋巴组织中淋巴细胞和抗原呈递细胞群体的组织情况。在第80天检测到了分泌免疫球蛋白和细胞因子的细胞。对胸腺、脾脏、淋巴结和肠黏膜进行了检测,以寻找表达CD3、CD5、CD20、CD68、p55和HLA - DR的细胞。在65日龄胎儿(妊娠中期早期)的脾脏中,绝大多数总淋巴细胞是CD5(+) CD20(+) B - 1细胞。其余淋巴细胞是CD3(+) T细胞。到第80天,脾脏中的B细胞和T细胞数量相等。65日龄胎儿的肠道中存在上皮内CD3(+) CD5(-) T细胞和固有层CD20(+) CD5(+) B细胞。到第80天,空肠和结肠中存在大量CD20(+) CD5(+) B细胞,早期淋巴细胞聚集形成明显。80至145日龄胎儿的脾脏中含有分泌免疫球蛋白M(IgM)的细胞,而分泌IgA、IgG、白细胞介素 - 6和γ干扰素的细胞在脾脏和结肠中大量存在。因此,到妊娠中期,恒河猴胎儿的淋巴组织拥有一套完整的、组织良好的抗原呈递细胞、T细胞和B细胞。

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